Function of the SRC-3 pathway in HSCs. SRC-3 is shown bound to the promoter region of the gene coding the acetyltransferase GCN5 in WT HSCs. CGN5 contributes to acetylate PGC-1α, thus inhibiting its cotranscriptional activity. This results in repression of the mitochondrial oxidative metabolism and maintenance of the quiescent state in HSCs. In SRC-3−/− HSCs, the deacetylation state of PGC-1α is shown to prevail because of the noncounteracted activity of sirtuins (SIRTs). In this state, PGC-1α can exert its transcriptional activity upregulating the expression of genes involved in mitochondrial biogenesis. This results in increased mass of mitochondria and mtDNA copy number, higher ΔΨm, and enhanced OCR, ROS generation, and ATP production. The phenotype of SRC-3−/− HSCs is characterized by loss of quiescence and lower long-term (LT) reconstitution capacity. These latter features in SRC-3−/− HSCs are prevented by treatment with the antioxidant N-acetyl cysteine (NAC) suggesting the involvement of ROS-mediated signaling. NRFs, nuclear respiratory factors; TFAM, mitochondrial transcription factor A.

Function of the SRC-3 pathway in HSCs. SRC-3 is shown bound to the promoter region of the gene coding the acetyltransferase GCN5 in WT HSCs. CGN5 contributes to acetylate PGC-1α, thus inhibiting its cotranscriptional activity. This results in repression of the mitochondrial oxidative metabolism and maintenance of the quiescent state in HSCs. In SRC-3−/− HSCs, the deacetylation state of PGC-1α is shown to prevail because of the noncounteracted activity of sirtuins (SIRTs). In this state, PGC-1α can exert its transcriptional activity upregulating the expression of genes involved in mitochondrial biogenesis. This results in increased mass of mitochondria and mtDNA copy number, higher ΔΨm, and enhanced OCR, ROS generation, and ATP production. The phenotype of SRC-3−/− HSCs is characterized by loss of quiescence and lower long-term (LT) reconstitution capacity. These latter features in SRC-3−/− HSCs are prevented by treatment with the antioxidant N-acetyl cysteine (NAC) suggesting the involvement of ROS-mediated signaling. NRFs, nuclear respiratory factors; TFAM, mitochondrial transcription factor A.

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